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AAV Gene Therapy for MPS1-associated Corneal Blindness.

Sci Rep. 2016; 
VanceMelisa,LlangaTelmo,BennettWill,WoodardKenton,MurlidharanGiridhar,ChungfatNeil,AsokanAravind,GilgerBrian,KurtzbergJoanne,SamulskiR Jude,HirschMatth
Products/Services Used Details Operation
Codon Optimization … The plasmid containing the intended AAV genome was first constructed by substituting the egfp gene in pTR-CMV-eGFP with the codon optimized IDUA cDNA (provided by GenScript) at the AgeI and SalI sites (now called pTR-CMV-opt-IDUA), or the wild type full-length hIDUA … Get A Quote

摘要

Although cord blood transplantation has significantly extended the lifespan of mucopolysaccharidosis type 1 (MPS1) patients, over 95% manifest cornea clouding with about 50% progressing to blindness. As corneal transplants are met with high rejection rates in MPS1 children, there remains no treatment to prevent blindness or restore vision in MPS1 children. Since MPS1 is caused by mutations in idua, which encodes alpha-L-iduronidase, a gene addition strategy to prevent, and potentially reverse, MPS1-associated corneal blindness was investigated. Initially, a codon optimized idua cDNA expression cassette (opt-IDUA) was validated for IDUA production and function following adeno-associated virus (AAV)... More

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